Piperidinesulfonylurea derivatives

ABSTRACT

A SERIES OF NOVEL 1-PIPERIDINESULFINYLUREA COMPOUNDS DERIVED FROM A NITROGEN-CONTAINING MONOCARBOXYLIC ACID HAVE BEEN PREPARED BY REACTING AN APPROPRIATE SULFAMIDE WITH AN ORGANIC ISOCYANATE OR A TRISUBSTITUTED UREA EQUIVALENT THEREOF. THE SULFAMYLUREAS SO OBTAINED ARE USEFUL IN THERAPY AS ORAL HYPOGLYCEMIC AGENTS. TYPICAL MEMBERS INCLUDES THOSE COMPOUNDS DERIVED FROM 2-METHOXYNICOTINIC ACID, OF WHICH 1-(BICYCLO(2.2.1)HEPT-5-EN-2-YL-ENDOMETHYL) -3- (4-(2-(2-METHOXYNICOTINAMIDO)ETHYL)-1-PIPERIDINESULFONYL)-UREA IS A MOST PREFERRED EMBODIMENT.

States Patent O 3,829,434 PIPERIDINESULFONYLUREA DERIVATIVES George R. Evanega, 'Ledyard, Donald E. Kuhla, Gales Ferry, and Reinhard Sarges, Mystic, Conn., assignors to Pfizer Inc.,'New York, N.Y. No Drawing. Filed Nov. 10, 1972, Ser. No. 305,594 a Int. Cl. C07d 31/50 U.S.- Cl.-260293.56 Claims ABSTRACT OF THE DISCLOSURE BACKGROUND OF THE INVENTION This invention relates to new and useful sulfamylurea derivatives, which are eifective in reducing blood sugar levels to a remarkably high degree. More particularly, it is concerned with certain novel 4-substituted-l-piperidinesulfonylureas and their base salts with pharmacologically acceptable, cations, which are useful in therapy as oral hypoglycemic agents for the treatment of diabetes.

In the past, various attempts have been made by numerous investigators in the field of organic medicinal chemistry to obtain new and better oral hypoglycemic agents. For the most part, these efforts have principally involved the synthesis and testing of various new and heretofore unavailableorganic compounds, particularly in the area of the sulfonylureas. However, in the search for still newer andmore improved oral hypoglycemic agents, far less is known about the activity of various heterocyclic sulfonylureas-like 4-substituted 1 piperidinesulfonylureas and their derivatives. For instance, I. M. McManus et al. in the Journal of Medicinal Chemistry, Vol. 8, p. 766 (1965) report .onseveral cyclicsulfamylureas that are active, but none of these compounds possess'any outstanding clinical advantages over that'of either chlorpropamide or tolbutarnide when used in this connection.

SUMMARY OF THE INVENTION RCONHGH CIL-CEW-SOgNHCONHR' andihe base salts. thereof with pharmacologically acceptable cations, wherein R. is. a member selected from the group consisting of' 2-methoxy-3-pyridyl, 2-ethoxy-3-pyridyl, 4 chloro-2.-.pyridyl and -8-quinolinyl, and R is amember selected from-the group consisting of bicyclo- [2.2.1]hept-S-en-Z-yLendo-methyl, bicyclo [2.2.1 ]hept-2- yl-endo-methyl, 7-oxabicyclo [2.2. l hept-Z-ylmethyl, l-adamantyl -and cycloalkylhaving from fiveto eight carbon atoms. These compounds are-all useful in lowering blood sugar levels when administered by the .oral route of administration. v t

4 3,829,434 Patented Aug. 13, 1974 Of special interest in this connection are such typical and preferred member compounds of the invention as 1- (bicycle [2.2. 1 hept-5-en-2-yl-end0-methyl) -3-{4- [2- (Z-methoxynicotinamido ethyl] l-pip eridinesulfonyl}urea, l-(bicyclo[2.2.1]hept-2-yl-end0-methyl-3-{4-[2-(2- methoxynicotinamido) ethyl] -1-piperidinesul fony1}urea, 1-(7-oxabicyclo[2.2.1]hept-Z-yl-endo-methyl)-3- {4- [2- Z-methoxynicotinamido) ethyl] l-piperidinesulfonyl}urea, 1-(7-oxabicyclo[2.2.1]hept-Z-yl-exo-methyl)-3-{4-[2- (2-methoxynicotinamido ethyl] l-piperidinesulfonyl}urea, l-bicyclo[2.2.1]hept-S-en-Z-yI-endo-methyl)-3-{4-[2- (4-chloropicolinamido ethyl] l-piperidinesulfonyl}urea, l-bicyclo[2.2.1]hept-5-en-2-yl-end0-methyl)-3-{4-[2- 8-quinolinecarboxamido ethyl] piperidinesulfonyl}urea and 1-cyclohexyl-3-{4- [2- 8-quinolinecarboxamido ethyl] l-pip eridinesulfonyl}ure a,

and their corresponding sodium salts. These particular compounds are all highly potent as regards their hypoglycemic activity.

DETAILED DESCRIPTION OF THE INVENTION In accordance with the process employed for preparing the novel compounds of this invention, an appropriately substituted sulfamide compound of the formula:

is reacted with an organic isocyanate reagent of the formula RNCO wherein R corresponds to the previously defined l-substituent on the urea moiety of the desired final product. In this way, the corresponding l-piperidinesulfonylurea compound is formed where R is defined as previously indicated. This particular reaction is normally conducted in a basic solvent medium, most desirably employing an aprotic organic solvent such as tetrahydrofuran, dimethylsulfoxide or dimethylformamide and preferably using a slight excess in moles of a base, like triethylamine or sodium hydride (in mineral oil), which may then be admixed with the solvent. Many of the aforesaid isocyanate reagents (RNCO) are either known compounds or else they can easily be prepared, using methods well-known to those skilled in the art, starting from readily available materials. In practice, it is usually preferable to employ at least about a molar equivalent of the isocyanate reagent in the aforesaid reaction of the present invention, with best results often being achieved by using a slight excess of same. Although any temperature below that of reflux may be used in order to effect the reaction, it is normally found most convenient in practice to employ elevated temperatures so as to shorten the required reaction time, which may range anywhere from several minutes up to about 24 hours depending, of course, upon the particular l-piperidinesulfonylurea actually being prepared. Upon completion of the reaction, the product is easily recovered from the spent reaction mixture in a conventional manner, e.g., by pouring same into an excess of ice-water containing a slight excess of acid, such as hydrochloric acid, whereby the desired l-piperidinesulfonylurea readily precipitates from solution and is subsequently collected by such means as suction filtration and appropriate 1,1,3-trisubstituted urea of the formula (R") NCONHR', wherein R" is an aryl group such as phenyl, p-chlorophenyl, p-bromophenyl, p-nitrophenyl, pacetylaminophenyl, p-tolyl, p-anisyl, u-naphthyl, B-naphthyl, and the like. This reaction is preferably carried out in the presence of a neutral polar organic solvent medium. Typical organic solvents for use in this connection include the N,N-dialkyl lower alkanoamides like dimethylformamide, dimethylacetamide, diethylformamide and diethylacetamide, as well as lower dialkyl sulfoxides such as dimethyl sulfoxide, diethyl sulfoxide and di-n-propyl sulfoxide, etc. It is desirable that the aforesaid solvent for this reaction be present in sufficient amount to dissolve each of the previously mentioned starting materials. In general, the reaction is conducted at a temperature that is in the range of from about 20 C. up to about 150 C. for a period of about one-half to about ten hours. The relative amounts of reagents employed are such that the molar ratio of 1- piperidinesulfamide to the 1,1-diaryl-3-(monosubstituted) urea is most desirably in the preferred range of from about 1:1 to about 1:2, respectively. Recovery of the desired product from the reaction mixture is then achieved by first diluting the reaction solution with water and then adjusting if necessary the pH of the resulting solution to a value of at least about 8.0, followed by subsequent extraction of the basic aqueous solution with any water-immiscible organic solvent in order to remove the diarylamine byproduct of formula (R") NH as well as minor amounts of unreacted or excess starting material that might possibly be present at this stage. Isolation of the desired l-piperidinesulfonylurea from the basic aqueous layer then follows in due course, viz., by adding a sufficient amount of a dilute aqueous acid solution to cause precipitation of the desired sulfamylurea to occur.

The two major type starting materials required for this reaction, viz., the l-piperidinesulfamides and the 1,1-diaryl-3-(monosubstituted)ureas, are both readily prepared by those skilled in the art in accordance with the conventional methods of organic chemistry. For instance, the 1- piperidinesulfamides, which are novel compounds and are also used as starting materials in the previously described isocyanate method, are suitably obtained by using classical methods of synthesis starting from the known 4-(2- aminoethyl)pyridine and proceeding in accordance with standard organic procedure as hereinafter described in the experimental section of this specification in some detail (see Preparations A-D and Examples I-IV). The 1,1-diaryl-3-(monosubstituted)-ureas, on the other hand, are all readily prepared from common organic reagents by employing standard procedures well known in the art, e.g., the desired 1,1,3-trisubstituted urea may be prepared from the corresponding disubstituted carbamyl chloride and the appropriate amine (R'NH in accordance with the general procedure of J. F. L. Reudler, as described in Recueil des T ravaux Chimiques des PaIys-Bas, Vol. 33, p. 64 1914).

The chemical bases which are used as reagents in this invention to prepare the aforementioned pharmaceutically acceptable base salts are those which form non-toxic salts with the many herein described acidic l-piperidinesulfonyl ureas, such as 1-(bicyclo[2.2.1]hept-S-en-2-yl-end0-methyl)-3-4-[2-(Z-methoxynicotinamido)ethyl] 1- piperidinesulfonyl urea, for example. These particular non-toxic base salts are of such nature that their cations are said to be essentially non-toxic in character over the wide range of dosage administered. Examples of such cations include those of sodium, potassium, calcium and magnesium, etc. These salts can easily be prepared by simply treating the aforementioned 1-piperidinesulfonylureas with an aqueous solution of the desired pharmacologically acceptable base, i.e., those oxides, hydroxides or carbonates which contain pharmacologically acceptable cations, and then evaporating the resulting solution to dryness while preferably bemg placed under reduced pressure. Alternatively, they may also be prepared by mixing lower alkanolic solutions of the said acidic compounds and the desired alkali metal alkoxide together, and then evaporating the resulting solution in the same manner as before. In either case, stoichiometric amounts of reagents must. be employed in order to ensure completeness of reaction and maximum production of yields with respect to the desiredfinal product."

As previously indicated, the l-piperidinesulfonylurea compounds of this invention are allreadily'- adapted to therapeutic use as oral hypoglycemic agents, in view of their ability to lower the bloodsugar levels of diabetic and non-diabetic subjects to a statistically significant degree. For instance, 1-bicyclo[2.2.1 hept-5-en-2-yl-endomethyl-3-{4-[2-(2-methoxynicotinamido)ethyl] 1 piper idinesulfonyl}urea (as the sodium salt), a typical'and preferred agent of the present invention, has been found to consistently lower blood sugar levels in the normal fasted rat (as well as infed rats and dogs) to a statistically significant degree when given bythe intraperitoneal route of administration at close levels'ranging from 1.0 gm./ kg. to 15 mg./kg., respectively, without showing any substan tial signs of toxic side effects. The other compounds of this invention also cause similar side effects. Furthermore, all the herein described compounds of this invention can be administered orally, for the present purposes at hand, without causing any significant untoward pharmacological side reactions to occur in the subject to whom they are so administered. In general, these compounds are ordinarily administered at dosage levels ranging from about 0.1 mg. to about 2.5 mg. per kg. of body weight per day, although variations will necessarily occur depending upon the condition and individual response of the subject being treated and the particular type of oral formulation chosen;

In connection with the use of the l-piperidinesulfonylurea compounds of this invention for the treatment of diabetic subjects, it is to be noted that they may be administered either alone or in combination with pharma ceutically acceptable carriers and that such administration can be carried out in both single and multiple dosages.

More particularly, the novel compounds of the invention can be administered in a wide variety of different dosage forms, i.e., they may be combined with various pharmaceutically acceptable inert carriers in the form of tablets, capsules, lozenges, troches, hard candies, powders, aqueous suspension, elixirs, syrups and the like; Such carriers include solid diluents or fillers, sterile aqueous media and various non-toxic organic solvents, etc. Moreover, such oral pharmaceutical compositions can be suitably sweetened and/or flavored by means of various agents of the type commonly employed for just such a purpose. In general, the therapeutically-effective compounds of this invention are present in such dosage forms at concentration levels ranging from about 0.5% to about by Weight of the total composition, i.e., in amounts'which aresufficient to provide the desired unit dosage.

For purposes of oral administration, tablets containing various excipients such as sodium citrate, calcium carbonate and dicalcium phosphate may be employed along with various disintegrants such as starch and preferably potato or tapioca starch, alginic acid and certain complex sllicates, together with binding agents such as polyvinylpyrrolidone, gelatin and acacia. Additionally, lubricating agents such as magnesium stearate, sodium lauryl sulfate and talc are often very useful for tabletting purposes. Solid compositions of a similar type may also be employed as fillers in soft and hard-filled gelatin capsules: preferred materials in this connection would also include the high molecular weight polyethylene glycols. When aqueous suspensions and/or elixirs are desired for oral admi nistra tion, the essential active ingredient therein may'be com bined with various sweetening or flavoring agents, coloring matter or dyes and, if so desired, ernulsifying and/ orj suspending agents as well, together with such diluents as water, ethanol, propylene glycol, glycerin and various like combinations thereof.

The activity of the compounds of the present invention, as hypoglycemic agents, is determined by their ability to lower blood sugar levels in the normal fasted rat when tested therein for such purposes according to the procedure described by W. S. Hoffman, as reported in the Journal of Biological Chlemistry, Vol. 120, p. 51 (1937). The latter method measures directly the amount of glucose in the blood at any given time and from this, the maximum percent decrease in blood sugar can be readily calculated and reported as hypoglycemic activity per se. In this-way, the present l-piperidinesulfonylurea compounds are shown to markedly reduce the blood sugar levels of non-anesthetized rats when administered to them at dose levels as low as 1.0 mg./kg.

Preparation A To a rapidly-stirred solution consisting of 148.1 g. (1.0 mole) of phthalic anhydride dissolved in 1000 ml. of xylene and also containing 13 ml. of triethylamine, there was slowly added in a dropwise manner 122.1 g. (1.0 mole) of 4-(2-aminoethyl)-pyridine [L. E. Brady et al., Journal of Organic Chemistry, Vol. 26, p. 4758 (1961)] dissolved in 1000 ml. of xylene. The reaction was slightly exothermic in nature and a heavy orange-yellow gum was observed to precipitate from the stirred system toward the end of the addition step. Upon completion of the addition, the resulting reaction mixture was refluxed for a period of approximately two hours (using a Dean-Stark trap to remove the water therefrom) and there was thus obtained a completely homogeneous yellow liquid. The latter liquid was then decanted while still hot into a 2- liter Erlenmeyer flask and slowly allowed to crystallize on cooling to room temperature (-25 C.). In this manner, therewere ultimately obtained 209 g. (83%) of crystalline 4-(2-phthalimidoethyl) pyridine in the form of a white solid material melting at 155157 C.

Anal.-Calcd. for C15H18N2O2I C, H, N, 11.11. Found: C, 71.55; H, 4.91; N, 10.75.

A 15-gal. autoclave was charged with 1.8 kg. (7.13 moles) of 4-(2-phthalimidoethyl)pyridine, 10.62 gal. of anhydrous methanol saturated with dry hydrogen chloride gas and 72.2 g. of platinum oxide catalyst. The autoclave and its contents were then placed under 200 p.s.i. pressure of hydrogen, while at 50 C. and held at that point until 95% of the theoretical hydrogen uptake was complete (this required approximately 4.33 hours). At the end of this time, the reaction mixture was cooled to 24 C., vented and then purged with nitrogen. After removal of the catalyst by means of fil'tration, the resulting filtrate was concentrated in vacuo to a final volume of ca. 3.0 liters and the solid product, which had precipitated from the residual liquid during the course of the concentration step, was then recovered by means of collecting same on a filter funnel with the aid of suction filtration. Upon washing with isopropanol and air-drying to constant weight, there was obtained 1070 g. (51%) of crystalline 4-(2-phthalimidoethyl)piperidinehydrochloride in the form of a pure white solid (m.p. 235-242 C.). Recrystallization from ethanol-diethyl ether then raised the melting point to 240-242 C. (analytical sample).

Anal.Calcd. for C 'H N O -HCl: C, 61.07; H, 6.49; N, 9.50. Found: C, 60.79; H, 6.37; N, 9.43.

- lA 12-liter' three-necked, round-bottomed flask was charged with 1700 g. (5.69 mole) of 4-(2-phthalimidoethyl)piperidine hydrochlon'bde, 552 g. (5.69 mole) of sulfamide and 5.8 liters of pyridine. The resulting reaction mixture was then stirred under reflux conditions for a period of 24 hours and finally cooled to room temperature (-25 C.).. The cooled mixture was next poured into an ice-watermixture (36 liters) and stirred for an additional period of 30 minutes. At this point, the precipitated product was collected '-by means of suction filtration, washed with 5.0 liters of 0'.'1N hydrochloric acid, then with 15 liters of water and finally with 3.0 liters of cold ethanol. After air-drying to constant weight, there was obtained a 1326 g. (71%) yield of pure 4-(2-phthalimidoethy1)-1- piperidinesulfonamide, m.p. 195197 C. Recrystallization from ethanol then gave the analytical sample as a white solid material (m.p. 202-203 C.).

A l-liter round-bottomed flask was charged with 28.4 g. (0.084 mole) of 4-(2-phthalimidoethyl)-1-piperidinesulfonamide, 2.7 g. (0.084 mole) of anhydrous hydrazine and 250 ml. of methanol. The resulting white suspension was stirred and then refluxed for a period of minutes, following by removal of the most of the methanol via fractional distillation. At this point, the reaction mixture was observed to be a homogeneous yellow solution. Concentrated hydrochloric acid (350 ml.) was then added, and the resulting mixture was refluxed for an additional period of three hours before being cooled to room temperature. The insoluble byproduct, which appeared at this point as a precipitate, was then removed by means of suction filtration and the resulting filtrate was thereafter evaporated to near dryness while under reduced pressure to give a white solid material as the final residual product. The latter was subsequently triturated with hot acetone, filtered and air dried to constant weight to afford 18.5 g. (91%.) of pure 4-(2-aminoethy1)-lpiperidinesulfonamide hydrochloride, m.p. 188-192 C. Recrystallization from ethanol then gave the analytical sample (m.p. 195l97 C.).

Anal.Calcd. for C H N O S-HCl: C, 34.49; H, 7.44; N, 17.24. Found: C, 34.56; H, 7.45; N, 17.24.

Preparation B A stirred suspension consisting of 57 g. (0.362 mole) of 2-chloronicotinic acid [6. M. Badger et al., Australian Journal of Chemistry, Vol. 18, p. 1267 (1965)] in 800 ml. of methanol was treated portion-wise with 43 g. (0.797 mole) of sodium methoxide. The resulting turbid solution was then heated in an autoclave at C. for a period of 11 hours. The reaction mixture obtained in this manner was then evaporated to near dryness (while under reduced pressure) and the residue was subsequently dissolved in 2000 ml. of Water, filtered and the resulting filtrate thereafter acidified with 1000 ml. of glacial acetic acid. The acidified filtrate was then concentrated in vacuo to a volume of ca. 800 ml., cooled in an ice bath for a period of approximately one hour and the resulting crystalline crop (i.e., precipitate) thereafter collected by means of suction filtration. After air drying to constant weight, there was obtained 33.3 g. (60%) of final product melting at 143146 C. Crystallization of the latter material from ml. of acetonitrile then gave 27.6 g. (50%) of pure 2-methoxynicotinic acid, m.p. 144-146 C. [literature m.p. 144146 C., according to Chemical Abstracts, Vol.68, p. 12876g (1968)].

To a suspension of 256 g. (1.675 mole) of 2-methoxynicotinic acid in 5.0 liters of methylene chloride, there were added 1000 ml. of thionyl chloride in one portion and the resulting reaction mixture was then heated on a steam bath to the reflux temperature. After a period of two hours at the reflux point, the clear solution was cooled and then concentrated in vacuo at room temperature to afford a residual oil. The excess thionyl chloride present was next removed by adding 500 ml. of benzene and subsequently evaporating the mixture to dryness while under reduced pressure. This particular purification step was then repeated twice and there was ultimately obtained 288 g. of pure Z-methoxynicotinoyl chloride as the residue, which solidified on standing and was used as such in the next reaction step. The yield of product was nearly quantitative.

Preparation C v The procedure described in Preparation B is repeated except that sodium ethoxide is the reagent of choice employed instead of sodium methoxide. In this particular case, using the same molar proportions as before, 2-chloronicotinic acid is converted to 2-ethoxynicotinic acid in a most facile manner. Treatment of the latter material with an excess of thionyl chloride then yields 2-ethoxynicotinoyl chloride.

Preparation D A suspension of 1.26 g. (0.008 mole) of 4-chloropicolinic acid [H. Meyer et al., Chemische Berichte, Vol. 61, p. 2210 (1928)] in 10 ml. of thionyl chloride was refiuxed on a steam bath until the evolution of hydrogen chloride and sulfur dioxide gas both ceased. Excess thionyl chloride was then removed by means of evaporation under reduced pressure and there was ultimately obtained pure 4-chloropicolinoyl chloride as a white residual solid, which was used as such in the next reaction step without any further purification being necessary. The yield of product obtained in this manner was almost quantitative.

Preparation E A 500 ml. three-necked, round bottomed flask was charged with 14.6 g. (0.119 mole) of endo-Z-aminoethylbicyclo[2.2.1]hept-5-ene [P. Wilder et al., Journal of rganic Chemistry, Vol. 30, p. 3078 (1965)], 18.0 g. (0.178 mole) of triethylamine and 100 ml. of tetrahydrofuran. The mixture was then rapidly cooled and stirred in an ice bath, while a solution consisting of 27.4 g. (0.119 mole) of N,N-diphenylcarbamoyl chloride dissolved in 100 ml. of tetrahydrofuran was slowly added thereto in a dropwise manner. After the addition was complete, the reaction mixture was stirred at room temperature (-25 C.) for a period of one hour and the resulting solution was then concentrated in vacuo (to approximately onethird of its original volume) to remove most of the tetrahydrofuran. On cooling, there was obtained a crystalline precipitate, which was subsequently collected by means of suction filtration and thereafter suspended in 250 ml. of 1N aqueous hydrochloric acid. Extraction of the latter aqueous solution with three 200-ml. portions of chloroform, followed by drying of the combined organic extracts then gave a clear organic solution upon filtration. After evaporating the clear filtrate to near dryness while under reduced pressure, there was ultimately obtained a heavy viscous oil, which subsequently crystallized on trituration with n-hexane. Recrystallization of this latter material from diethyl ether/n-hexane then gave pure 1,1-diphenyl- 3-(bicyclo[2.2.1]hept-5-en-2-yl-endo methyl)urea, m.p. 129130 C. The analytical sample was a crystalline white solid.

Anal.--Calcd. for C H N O: C, 79.21; H, 6.96; N, 8.80. Found: C, 79.19; H, 7.05; N, 8.93.

Preparation F A 3-liter round-bottomed flask was charged with 212 g. (4.0 moles) of acrylonitrile, 272 g. (4.0 moles) of furan and 50 mg. of hydroquinone all dissolved in a total of one liter of dry benzene. Stirring was then commenced, while a solution consisting of 55 ml. (0.5 mole) of titanium tetrachloride dissolved in 500 ml. of benzene was added at such a rate that the temperature did not exceed 35 C. The resulting mixture was then stirred at room temperaure (-25 C.) for a period of five days in order to complete the reaction, followed by treatment with 500 ml. of 0.5N hydrochloric acid. After filtering the acidified mixture, the benzene layer was collected and subsequently saved, while the aqueous layer was extracted anew with a fresh portion of benzene. At this point, the organic layers were combined, washed with water and then dried over anhydrous magnesium sulfate. After removal of the drying agent by means of suction filtration and the organic solvent by means of evaporation under reduced pressure, there was obtained 156.3 g. (32%) of 7 oxabicyclo [2.2.1]hept--en-2-ylnitrile in the form of a crude mixture of endoand exo-isomers.

The above crude mixture (130 g.) was then hydrogenated in 1000 ml. of acetone at 50 p.s.i. pressure, using 2 g. of palladium-on-barium sulfate as catalyst. After removal of the catalyst by means of suction filtration and the solvent by means of evaporation under reduced pressure, there was obtained a residual liquid which on fractional distillation gave 55.5 g. (42%) of pure ndo-7- oxabicyclo[2.2.1]hept-2-ylnitrile (b.p. 45 C./0.1 mm. Hg) and 37.9 g. (29%) of pure ex0-7-oxabicyclo[2.2.1]- hept-2-ylnitrile (b.p. 48 C./0.02 mm. Hg), plus 14.7 g. (11%) of an endo/exo mixture. I

Anal.Calcd. for C H NO: C, 68.27;"H, 7.37; N, 11.37. Found: (endo): C, 67.96; H, 7.21;N, 11.37; (2x0): C, 68.32; H, 7.42; N, 11.64.

To a well-stirred solution consisting of 54.3 g. (0.44 mole) of endoJ-oxabicyclo[2.2.1]hept 2-ylnitrile dissolved in 500 ml. of methanol, there were added 24 ml. of a slurry of Raney nickel in methanol, followed by the dropwise addition of 33.2 g. (0.88 mole) of sodium borohydride dissolved in 110 ml. of 4N aqueous sodium hydroxide. The latter step was carried out with the aid of external cooling so as to keepthe temperature of the reaction mixture within the 40-50 C. range. Afterfthe addition .was complete (and this required approximately 25 minutes), the mixture was further stirred at ambient temperature (i.e., without cooling) for a period of 20 minutes, at which point no further gas evolution could be detected. The spent reaction mixture was then filtered to remove solid impurities, and the resulting filtrate thereafter concentrated in vacuo to afford a residue. that was subseqeuntly suspended in 500 ml. of 1N aqueous sodium hydroxide. After extracting the latter basic aqueous solution three times with chloroform, the chloroform extracts were combined, dried over anhydrous magnesium sulfate and thereafter evaporated to constant volume while under reduced pressure to give 55.5 g. (100%) of end0-7-oxabicyclo[2.2.1]hept-2-ylmethylamine (b.p. C./10 mm. Hg), which was used as such in the next reaction step without any further purification being necessary.

The procedure described in Preparation E was now repeated to prepare the 1,1-diphenyl-3-(monosubstituted) urea compound except that end0-7-oxabicyclo[2.2.1] hepta-2-ylmethylamine obtained as described above was the appropriate amine starting material employed in place of end0 2-amin0methylbicycl0[2.2.1]hept-S-ene, again using the same molar proportions as before. In this particular case, the corresponding final product thus. obtained was 1,1-diphenyl-3-(7-oxabicyclo[2.2.1]hept-2- yl-endo-methyDurea, m.p. 109-1 11 C.

AnaL-Calcd. for C H N O C, 74.49; H, 6.89; N, 8.68. Found: C, 74.28; H, 6.93; N, 8.61.

Preparation G A methanolic solution of the exo-nitrile compound prepared as described in Preparation F was treatedin exactly the same manner as that previously described for the corresponding endo-isomer, with respect to Raney nickel and sodium borohydride reduction. In this Way, pure exo-7-oxabicyclo[2.2.1]hept-2-ylnitrile was converted to ex0-7-oxabicyclo-[2.2.1]hept-2-ylmethylamine in substantially high yield. The latter material was used as such in the next reaction step without any further purification being necessary. i

The procedure described in Preparation E was repeated once again to prepare the desired 1,1-diphenyl-3-(monosubstituted)urea compound except that this time exo-7'- oxabicyclo[2.2.1]hept-2-ylmethylamine was 1 the starting material employed in place of endmZ-aminomethylbicy clo[2.2.1]hept-5-ene, albeit on the same molar basis as before. In this particular case, the corresponding final product thus obtained was 1',1-diphenyl-3-(7-oxabicy-= Example I A solution consisting of 286.5 g. (1.67 moles) of 2- methoxynicotinoyl chloride dissolved in 2.0 liters of chloroform and a solution of 530 g. (5.0 moles) of sodium carbonate in 2225 ml. of water were added simultaneously at the rate of 25 mL/minute to 407 g. (1.67 moles) of 4- (2-aminoethyl)-l-piperidinesulfonamide hydrochloride dissolved in 2.75 liters of Water, which also contained 177 g. (1.67 moles) of sodium carbonate. Vigorous agitation was maintained throughout the addition step. after which the reaction mixture was then further stirred at room temperature (-25 C.) for 1.5 hours. At this point, the precipitated solids which formed were subsequently recovered by means of suction filtration and thereafter washed with two separate-500 ml. portions of cold acetone. After air-drying to constant weight, the yield of crude material amounted to 630 g. of product melting at 165-172 C. Recrystallization from 12.5 liters of acetonitrile then gave' 409 g. (71%) of pure 4-[2-(2-methoxynicotiuamido)ethyl]-l-piperidinesulfonamide, m.p. 182- 183 C.

Anal.'Calcd.for C H N S C, 49.11; H, 6.48; N, 16.37. Found: C, 49.24; H, 6.46; N, 16.42.

Example II The procedure described in Example I is repeated using 2-ethoxynicotionyl chloride in place of 2-methoxynicotinoyl chloride on the same molar basis as before. In this particular case, the corresponding final product thus obtained is 4-[2-(2-ethoxynicotinamido)ethylJ-l-piperidinesulfonamide.

Example III To a mixture of 1.95 g. (0.008 mole) of 4-(2-aminoethyl)1-piperidinesulfonamide hydrochloride and 2.22 ml. (0.016 mole) of triethylamine in ml. of dry tetrahydrofuran, there were added 1.41 g. (0.008 mole) of 4-chloropicolinoyl chloride dissolved in 15 ml. of tetrathermic (-40 C.) and after completion was slightly exothermc (-40 C.) and after completion of same, the resulting reaction mixture was stirred at ambient temperatures for a period of approximately 16 hours. At this point, the thoroughly stirred mixture was poured into 50 ml. of ice water and subsequently acidified with a few drops of 3N aqueous hydrochloric acid. The resulting crystalline precipitate was then recovered by means of suction filtration and thereafter recrystallized twice from acetonitrile to afford 0.997 g. of pure product. In this way, there was ultimately obtained a 36% yield of 4- [2-(4 chloro-picolinamido)ethyl] l-piperidinesulfonamide, m.p. 186187 C.

AnaL-Calcd. for C H CIN O S: C, 45.00; H, 5.52; N, 16.6. Found: C, 45.21; I-I, 5.38; N, 16.19.

Example IV In 51150 I111. three-necked, round bottom flask equipped with mechanical stirrer, reflux condenser and heating mantle, there were placed 3.0 g. (0.0173 mole) of quinoline- 8-ca'rboxylic acid, 8.1 g. (0.0327 mole) of N-ethoxycarbonyl-2-ethoxycarbonyl-2 'ethoxy-1,3-di.hydroquinoline (EEDQ), 3.82 g. (0.01635 mole) of 4-(2-aminoethyl)-l-piperidinesulfonamide hydrochloride and 1.66 g. (0.01635 mole) of'triethylamine' all in a total of 50 ml. of tetrahydrofuran. Stirring was commenced and the resulting mixture was heated under reflux for a period of approximately 16'hours. At the end of this time, the re action'mixture was cooled to room temperature C.) and the dilutedwith 200 ml. of chloroform prior to extraction with two 100 ml. portions of 2N aqueous sodium hydroxide. The aqueous extracts so obtained were combined and then re-extracted once'with 75 ml. of chloroform prior to being adjusted to a pH value of ca. 7.0 via the slow addition of 2N aqueous hydrochloric acid solution thereto. The desired product precipitated at this point, as a gummy white solid, which was collected and 10 thereafter recrystallized from methanol to afford 3.8 g. (63%) of pure 4-[2-(8-quinolinecarboxamido)ethyl]- l-piperidinesulfonamide, m.p. 205.5-206.5 C.

AnaL-Calcd. for C H N O S- /2H O: C, 54.96; H, 6.23; N, 15.08. Found: C, 55.37; H, 6.38; N, 14.80.

Example V To a solution consisting of 407 g. (1.19 mole) of 4-[2- (2-methoxynicotinamido)ethyl]-1 piperidinesulfonamide and 380 g. (1.19 moles) of 1,1-diphenyl-3-(bicyclo[2.2.1]

,hept-5-en-2-yl-endo-methyl)urea dissolved in 3.0 liters of dry N, N-dimethylformamide, there were added 51 g. 1.19 moles) of 56% sodium hydride (in mineral oil) in one full portion. The resulting reaction mixture was then heated to 65 C., at which point it became slightly exothermic and the temperature rose to 70 C. After a period of stirring for 20 minutes, a homogene ous solution was formed and the latter was subsequently poured into two volumes of diethyl ether, followed by extraction with one volume of water and acidification of the aqueous layer with 6N hydrochloric acid. After extracting the latter solution with one volume of ethyl acetate, the organic layer was decolorized with charcoal and then dried over anhydrous magnesium sulfate. Upon removal of the drying agent by means of suction filtration and the solvent by means of evaporation under reduced pressure, there was ultimately obtained a viscous oil, which was subse quently dissolved in one liter of acetonitrile. The latter solution was filtered while hot, allowed to cool to room temperature and then slowly diluted with two liters of diethyl ether to give a pale yellow precipitate, which was subsequently collected by means of suction filtration. The crystalline material so obtained was then air-dried to constant weight to give 374 g. (64%) of pure l-(bic-yclo [2.2.1]hept 5 en 2 y l endo methyl) 3 {4 [2- (2 methoxynicotinamid'o)ethyl] 1 piperidinesulfonyl} urea, m.p. 92 C.

Anal.--Calcd. for C22H25N505S: C, H, N 14.25. Found: C, 56.27; H, 6.96; N, 13.84.

Example VI A mixture of 983 mg. (0.002 mole) of 1-(bicyclo [2.2.1]hept 5 en 2 yl endo methyl) 3 {4 [2- (2 methoxynicotinamido)ethyl] 1 piperidinesulfonyl} urea in 50 ml. of tetrahydrofuran containing 50 mg. of 5% palladium-on-carbon catalyst was hydrogenated at 48 p.s.i. pressure for a period of 30 minutes. Upon completion of this step, the catalyst was removed by means of suction filtration and the resulting filtrate thereafter evaporated to near dryness while under reduced pressure to afford a white solid material as the crude residual product. After recrystallizing the latter material from acetonitrile, there was obtained 550 mg. (56%) of pure 1-(bicyclo[2.2.l] hept 2 yl endo methyl) 3 {4 [2 (2 methoxynicotinamido)ethyl]-1-piperidinesulfonyl}urea, m.p. 108 C.

Anal.Calcd. for C23H35N505S1 C, H, N, 14.19. Found: C, 56.10; H, 7.07; N, 14.16.

Example VII The procedure described in Example V was repeated except that 900 mg. (0.0026 mole) of 4-[2-(4-chloropicolinamido)ethyl]-1-piperidinesulfonamide and 930 mg. (0.0029 mole) of 1,1-diphenyl-3-(bicyclo) [2.2.1]hept-5- en-2-yl-endo-methyl)urea were reacted in 5.0 ml. of dry N,N-dimethylformamide in the presence of mg. (0.0029 mole) of 56% sodium hydride in mineral oil. The reaction mixture was heated at 60 C. for a period of 30 minutes, at which point thin-layer chromatography (TLC) analysis showed the conversion to be substantially complete. After pouring the mixture into ml. of anhydrous diethyl ether, the sodium salt of the product precipitated as a white gum. The ether was then decanted and the gum was subsequently dissolved in 20 ml. of water. Upon acidification with 5 .0 ml. of 3N hydrochloric acid and extraction into chloroform, followed by decolorization with charcoal and drying over anhydrous magnesium sulfate, there was obtained a clear chloroform solution of the desired product. Evaporation of the latter solution to complete dryness while under reduced pressure then gave 1.11 g. (86.5%) of pure 1-(bicyclo[2.2.1]hept-5-en-2-yl-endomethyl) 3 {4 [2 (4 chloropicolinamido)ethyl] 1- piperidinesulfonyl}urea as an amorphous solid material, m.p. 75-80 C.

AnaL-Calcd. for C H ClN O S: C, 53.27; H, 6.10; N, 14.12. Found: C, 53.11; H, 6.05; N, 13.89.

Example VIII The procedure described in Example V was repeated except that 1.0 g. (0.00276 mole) of 4-[2-(8-quinolinecarboxamido)ethyl] 1 piperidinesulfonamide and 879 mg. (0.00276 mole) of 1,1-diphenyl-3-(bicyclo[2.2.1]hept-5- en-Z-yl-endo-methyDurea were reacted in ml. of N,N- dimethylformamide in the presence of 118 mg. (0.00276 mole) of 56% sodium hydride (in mineral oil). In this manner, there was obtained a 210 mg. (14.7%) yield of pure 1 (bicyclo[2.2.l]hept-5-en-2-yl-endo-methyl)-3-{4- [2 (8 quinolinecarboxamido)ethyl] 1 piperidinesulfonyl}urea, m.p. 95 C. (decomp.).

Anal.Calcd. for C H N O S' /2H O: C, H, 6.58; N, 13.45. Found: C, 59.95; H, 6.43; N, 13.48.

Example IX The procedure described in Example V was repeated except that 500 mg. (0.00145 mole) of 4-[2-(2-methoxynicotinamido)ethyl1-l-piperidinesulfonamide and 218 mg. (0.00175 mole) of cyclohexyl isocyanate were reacted in 5.0 ml. of dry N,N-dimethylformamide in the presence of 75 mg. (0.00175 mole) of 56% sodium hydride (in mineral oil). In this manner, there was obtained a 310 mg. (38%) yield of 1-cyclohexyl-3-{4-[2-(2-methoxynic0tinamidoethyl-1-piperidinesulfonyl}urea, m.p. 173-175 C. after recrystallization from ethanol.

Anal.Calcd. for C H N O S: C, 53.94; H, 7.11; N, 14.98. Found: C, 53.72; H, 7.00; N, 14.88.

Example X The procedure described in Example V was repeated except that 500 mg. (0.00145 mole) of 4-[2-(2-methoxynicotinamido)ethyl]-1-piperidinesulfonamide and 316 mg. (0.0017 5 mole) of l-adamantyl isocyanate [H. Stetter et al., Chemische Berichte, Vol. 95, p. 2302 1962)] were reacted in 5.0 m1. of dry N,N-dimethylformamide in the presence of 75 mg. (0.00175 mole) of 56% sodium hydride (in mineral oil). In this manner, there was obtained a 250 mg. (33%) yield of pure 1-(1-adamantyl)-3-{4-[2- (2 methoxynicotinamido)ethyl] 1 piperidinesulfonyl} urea as a white solid material melting at 171-173 C.

AnaL-Calcd. for C H N O S: C, 57 .7-8; H, 7.18; N, 13.48. Found: C, 57.46; H, 7.09; N, 13.45.

Example XI The procedure described in Example V was repeated except that 1.0 .g. (0.00276 mole) of 4-[2-(8-quinolinecarboxamido)ethyl]-1-piperidinesulfonamide and 345 mg. (0.00276 mole) of cyclohexyl isocyanate were reacted in 10 ml. of dry N,N-dimethyl.formamide in the presence of 118 mg. (0.00276 mole) of 56% sodium hydride (in mineral oil). In this manner, there was obtained 820 mg. (61%) of pure 1-c-yclohexyl-3-{4-[2-(8-quinolinecarboxamido)ethyl]-1-piperidinesulfonyl}urea in the form of a white solid, m.p. 177-179 C. (decomp.) after recrystallization from acetonitrile.

Anal.Calcd. for C H N O S: C, 59.11; H, 6.82; N, 14.36. Found: C, 58.95; H, 6.78; N, 14.69.

Example XII The procedure described in Example V was repeated except that 190 mg. (0.00055 mole) of 4-[2-(2-methoxynicotinamido)ethyl] 1 piperidinesulfonamide and 225 mg. (0.0007 mole) of 1,2-diphenyl-3-(7-oxabicyclo[2.2.1] hept-2-yl-end0-methyl)urea were reacted in 5.0 ml. of N, N-dimethylformamide in the presence of 34 mg. (0.0007 mole) of 49% sodium hydride (in mineral oil). Thereaction mixture was then allowed to stand at room temperature (-25 C.) overnight (a period of approximately 16 hours) prior to work-up. In this manner, there was obtained a 154 mg. (57%) yield of pure 1-(7-oxabicyclo- [2.2.1]hept 2 yl-endo-methyl)-3-{4-[2-(2 methoxynicotinamido)ethyl] 1 piperidinesulfonyl}urea,- m.p. 109-110 C. I

Anal.-Calcd. for C22H33N506S: C, H, N, 14.13. Found: C, 53.09; H, 6.51; N, 13.88.

Example XIII Example XIV The following l-piperidinesulfonylureas are prepared by employing the procedures described in the previous examples, starting from the corresponding sulfamide and the appropriate organic isocyanate or 1,1-diphenyl-3-substituted urea in each instance:

2-methoxy-3-pyridyl. Cyclopentyl. Do Cycloheptyl. Do Cyclooetyl.

Z-ethoxy-B-pyndyl. Bicycl0[2.2.1 hept-S-en-Z-yI-endo-methyl. Do Bicyclo[2.2.1 hept-2-yl-endo-methyl. Do 7-oxabicyclol22.1}hept-2-yl-endo-methyl. Do 7-oxabioyclo[2.2.1 hept-2-yl-ezo-methyl.

Do.. l-adamantyl. Do Cyolopentyl. Do Cyclohexyl.

Oycloheptyl.

o Cyclooctyl.

4-chl0ro-2-pyridy Bicyclo[2.2.1]hept-2-yl-endo-methyl.

Do 7-oxabicyelo[2.2.1]hept-2-yl-endo-methyl: Do. 7-oxabicyclo[2.2.1]hept-2-yl-ezo-methyl. Do l-adamantyl. Do Cyelo entyl. Do Cyclo exyl. Do-. Cycloheptyl. Do Cyclooetyl.

S-quinolinyl Bieyclolz. .lEhept-2-yl-endo-methyl.

D 7-oxabieyclo 2.2.1%hept-2-yl-endo-methyl.

. 7-oxabicyclo[2.2.1 hept-Z-yl-ezo-methyl. l-adamantyl.

. Cyclopentyl.

.. Cycloheptyl.

Cyclooctyl.

Example XV A solution consisting of 354 g. (0.72 mole) of l-(bicyclo[2.2.1]hept 5 en-2-yl-end0-methyl)-3-{4 -[2-(2- methoxynicotinamido)ethyl] 1 piperidinesulfonyl}urea dissolved in 2.0 liters of methanol was treated at 0 C. with 38.9 g. (0.72 mole) of sodium methoxide divided into five separate portions. The reaction mixture was then concentrated in vacuo and the resulting residue thereafter recrystallized from 7.0 liters of acetonitrile to give a 353 g. yield of product, viz., the sodium salt of lf-(bi: cyclo[2.2.1]hept 5 en-2-yl-end0-methyl)-3-{4-[2-(2 methoxynicotinamido)ethyl] 1 piperidinesulfonyl}urea m.p. 208-210 C.

Anal.-Calcd. for C H N O SNa: C,.53.7 9;, H, 6.28; N, 13.64. Found: C, 53.54; H, 6.42; N, 13.40.,

Example XVI 1-piperidinesulfonyl}urea is prepared by dissolving said compound in anhydrous methanol and then adding said solution to another methanolic solution which contains an equivalent amount in moles of sodium methoxide. Upon subsequent evaporation of the solvent therefrom via freeze-drying, there is obtained the desired alkali metal salt in the form of an amorphous solid powder which is freely soluble in water.

In like manner, the potassium and lithium salts are also similarly prepared, as are the alkali metal salts of all the other acidic l-piperidinesulfonylureas of this invention which are reported in the previous examples.

Example XVII The calcium salt of 1-cyclohexyl-3-{4-[2-(8-quinolinecarboxamido)ethyl]-1-piperidinesulfonyl}urea is prepared by dissolving said compound in water containing an equivalent amount in moles of calcium hydroxide and then freeze-drying the mixture. The corresponding magnesium salt is also prepared in like manner, as are all the other alkaline-earth metal salts not only of this particular compound, but also of those acidic l-piperidinesulfonylureas previously described in Examples V-VIII and XXIV, respectively.

Example XVIII A dry solid pharmaceutical composition is prepared by blending the following materials together in the proportions by weight specified below:

1-(Bicyclo[2.2.1]hept en-2-yl-end0-methyl)-3- ,{4-[2 (2 methoxynicotinamido)ethyl1-l-piperidinesulfonyl}urea Sodium citrate 25 Alginic acid Polyvinylpyrrolidone 10 Magnesium stearate 5 After the dried composition is thoroughly blended, tablets are punched from the resulting mixture, each tablet being of such size that it contains 75 mg. of the active ingredient. Other tablets are also prepared in a similar fashion containing 5, 10, and 50 mg. of the active ingredient, respectively, by merely using the appropriate amount of the l-piperidinesulfonylurea in each case.

Example XIX A dry solid pharmaceutical composition is prepared by combining the following materials together in the proportions by weight indicated below:

l-Cyclohexyl 3 {4 [2-(8-quinolinecarboxamido) ethyl] 1 piperidinesulfonyl}urea 50 Calcium carbonate 20 Polyethylene glycol, average molecular weight, 4000 The dried solid mixture so prepared is then thoroughly agitated so as to obtain a powdered product that is completely uniform in every respect. Soft elastic and hardfilled gelatin capsule containing this pharmaceutical composition are then prepared, employing a sufficient quantity of material in each instance so as to provide each capsule with 125 mg. of the active ingredient.

Example XX The l-piperidinesulfonylurea final products of Examples V-XIII were tested for hypoglycemic activity in groups of six male albino rats (each weighing approximately 190-240 g.) of the Sprague-Dawley strain. No anesthetic was used in this study. The rats were fasted for approximately 18-24 hours prior to administration, a blood sample was then taken from the tail vein of each animal and the test compound was administered intraperitoneally (while in solution as the sodium salt in 0.9% saline) at dose levels of 15, 5.0 and 1.0 mg./kg., respectively. Additional blood samples were then taken at l, 2 and 4 hour intervals after administration of the Hypoglycemic acfgifigity (max. percent 1. 0 6. 0 l-piperidinesulfonylurea mgJkg. mgJkg.

Product of Example:

What is claimed is: 1. A sulfamylnrea compound selected from the group consisting of l-piperidinesulfonylureas of the formula:

and the base salts thereof with pharmacologically acceptable cations, wherein R is a member selected from the group consisting of 2-methoxy 3 pyridyl, 2-ethoxy-3- pyridyl and 4-chloro-2-pyridyl, and R is a member selected from the group consisting of bicyclo[2.2.1]hept-5- en 2 yl endo-methyl, bicyclo[2.2.1]hept-2-yl-end0- methyl, 7-oxabicyclo[2.2.l]hept 2 yl methyl, l-adamantyl and cycloalkyl having from five to eight carbon atoms.

2. A compound as claimed in Claim 1 wherein R is 2- methoxy-3-pyridyl.

3. A compound as claimed in Claim 1 wherein R is 4-chloro-2-pyridyl.

4. A compound as claimed in Claim 1 wherein R bicyclo[2.2.1]hept-5-en-2-yl-end0-methyl.

5. A compound as claimed in Claim 1 wherein R bicyclo[2.2.1]hept-Z-yl-endo-methyl.

6. A compound as claimed in Claim 1 wherein R 7-oxa-bicyclo[2.2.1]hept-Z-yl methyl.

7. A compound as claimed in Claim 1 wherein R cycloalkyl having from five to eight carbon atoms.

8. A compound as claimed in Claim 7 wherein R cyclohexyl.

9. 1-(Bicyclo[2.2.1]hept 5 en-2-yl-endo-methyl)-3- {4-[2-(2-methoxynicotinamido)ethyl] 1 piperidinesulfonyl}urea.

10. l-(7 Oxabicyclo[2.2.l]hept 2 yl-endo-methyD- 3-{4-[2 (2 methoxynicotinamido)ethyl]-1-piperidinesulfonyl}urea.

References Cited FOREIGN PATENTS 6/1971 West Germany. 11/1971 Japan.

G. THOMAS TODD, Primary Examiner US. Cl. X.R. 

